Your search keyword '"Richard Chahwan"' showing total 48 results

1. Intercellular Epigenomic Signalling via Extracellular Vesicles During B Cell Maturation

Author

Kevin Ho Wai Yim, Ala'a Al Hrout, and Richard Chahwan

Subjects

antibody maturation, extracellular vesicles, intercellular epigenomic signalling, non‐coding RNA, single particle analysis, Cytology, QH573-671

Abstract

ABSTRACT B cell maturation is crucial for effective adaptive immunity. It requires a complex signalling network to mediate antibody diversification through mutagenesis. B cells also rely on queues from other cells within the germinal centre. Recently, a novel class of intercellular signals mediated by extracellular vesicles (EVs) has emerged. Studies have shown that B cell EV‐mediated signalling is involved in immune response regulation and tumorigenesis. However, the mechanistic role of B cell EVs is not yet established. We herein study the biological properties and physiological function of B cell EVs during B cell maturation. We use emerging technologies to profile B cell EV surface marker signatures at the single particle level, molecular cargo and physiological roles in B cell maturation. EV ncRNA cargo, characterised by RNA‐seq, identified an EV‐mediated novel non‐coding RNA (ncRNA) regulatory network for B cell maturation. We show that a previously uncharacterised micro‐RNA (miR‐5099) in combination with a set of long ncRNA are carried within B cell EVs and could contribute to antibody diversification. The physiological role of EVs in B cell maturation is investigated using EV blockade assays and complementation studies using diverse EV sources further confirmed the physiological role and mode of action of EVs in B cell maturation.

Published

2025

2. DNA Methyltransferase Inhibition Upregulates the Costimulatory Molecule ICAM-1 and the Immunogenic Phenotype of Melanoma Cells

Author

Alessandra S.P. Cereghetti, Patrick Turko, Phil Cheng, Stephan Benke, Ala’a Al Hrout, Andreas Dzung, Reinhard Dummer, Michael O. Hottiger, Richard Chahwan, Lorenza P. Ferretti, and Mitchell P. Levesque

Subjects

DNA methyltransferase, DNMTi, Epigenetics, ICAM-1, Melanoma, Dermatology, RL1-803

Abstract

In cutaneous melanoma, epigenetic dysregulation is implicated in drug resistance and tumor immune escape. However, the epigenetic mechanisms that influence immune escape remain poorly understood. To elucidate how epigenetic dysregulation alters the expression of surface proteins that may be involved in drug targeting and immune escape, we performed a 3-dimensional surfaceome screen in primary melanoma cultures and identified the DNA-methyltransferase inhibitor decitabine as significantly upregulating the costimulatory molecule ICAM-1. By analyzing The Cancer Genome Atlas melanoma dataset, we further propose ICAM-1 upregulation on melanoma cells as a biomarker of a proinflammatory and antitumorigenic signature. Specifically, we showed that DNA-methyltransferase inhibitor administration upregulated the expression of the antigen-presenting machinery, HLA class I/II, as well as the secretion of the proinflammatory chemokines CXCL9 and CXCL10. Our in silico analysis on The Cancer Genome Atlas and ex vivo experiments on human primary melanoma samples revealed that increased ICAM-1 expression positively correlated with increased immunogenicity of human melanoma cells and correlated with increased immune cell infiltration. These findings suggest a therapeutic approach to modulate the immunogenic phenotype of melanoma cells, hence supporting the exploration of DNA-methyltransferase inhibitor as a potential inducer of infiltration in immunologically cold tumors.

Published

2025

3. Modelling liver cancer microenvironment using a novel 3D culture system

Author

Ala’a Al Hrout, Karla Cervantes-Gracia, Richard Chahwan, and Amr Amin

Subjects

Medicine, Science

Abstract

Abstract The tumor microenvironment and its contribution to tumorigenesis has been a focal highlight in recent years. A two-way communication between the tumor and the surrounding microenvironment sustains and contributes to the growth and metastasis of tumors. Progression and metastasis of hepatocellular carcinoma (HCC) have been reported to be exceedingly influenced by diverse microenvironmental cues. In this study, we present a 3D-culture model of liver cancer to better mimic in vivo tumor settings. By creating novel 3D co-culture model that combines free-floating and scaffold-based 3D-culture techniques of liver cancer cells and fibroblasts, we aimed to establish a simple albeit reproducible ex vivo cancer microenvironment model that captures tumor-stroma interactions. The model presented herein exhibited unique gene expression and protein expression profiles when compared to 2D and 3D mono-cultures of liver cancer cells. Our results showed that in vivo like conditions cannot be mimicked by simply growing cancer cells as spheroids, but by co-culturing them with 3D fibroblast with which they were able to crosstalk. This was evident by the upregulation of several pathways involved in HCC, and the increase in secreted factors by co-cultured cancer cells, many of which are also involved in tumor-stroma interactions. Compared to the conventional 2D culture, the proposed model exhibits an increase in the expression of genes associated with development, progression, and poor prognosis of HCC. Our results correlated with an aggressive outcome that better mirrors in vivo HCC, and therefore, a more reliable platform for molecular understanding of HCC.

Published

2022

4. Investigating the tumor-immune microenvironment through extracellular vesicles from frozen patient biopsies and 3D cultures

Author

Ala’a Al Hrout, Mitchell P. Levesque, and Richard Chahwan

Subjects

tumor microenvironment (TME), extracellular vesicle (EV), tumor immunity, immunotherapy, patient derived organoids, Immunologic diseases. Allergy, RC581-607

Abstract

Melanomas are highly immunogenic tumors that have been shown to activate the immune response. Nonetheless, a significant portion of melanoma cases are either unresponsive to immunotherapy or relapsed due to acquired resistance. During melanomagenesis, melanoma and immune cells undergo immunomodulatory mechanisms that aid in immune resistance and evasion. The crosstalk within melanoma microenvironment is facilitated through the secretion of soluble factors, growth factors, cytokines, and chemokines. In addition, the release and uptake of secretory vesicles known as extracellular vesicles (EVs) play a key role in shaping the tumor microenvironment (TME). Melanoma-derived EVs have been implicated in immune suppression and escape, promoting tumor progression. In the context of cancer patients, EVs are usually isolated from biofluids such as serum, urine, and saliva. Nonetheless, this approach neglects the fact that biofluid-derived EVs reflect not only the tumor, but also include contributions from different organs and cell types. For that, isolating EVs from tissue samples allows for studying different cell populations resident at the tumor site, such as tumor-infiltrating lymphocytes and their secreted EVs, which play a central anti-tumor role. Herein, we outline the first instance of a method for EV isolation from frozen tissue samples at high purity and sensitivity that can be easily reproduced without the need for complicated isolation methods. Our method of processing the tissue not only circumvents the need for hard-to-acquire freshly isolated tissue samples, but also preserves EV surface proteins which allows for multiplex surface markers profiling. Tissue-derived EVs provide insight into the physiological role of EVs enrichment at tumor sites, which can be overlooked when studying circulating EVs coming from different sources. Tissue-derived EVs could be further characterized in terms of their genomics and proteomics to identify possible mechanisms for regulating the TME. Additionally, identified markers could be correlated to overall patient survival and disease progression for prognostic purposes.

Published

2023

5. Serum extracellular vesicles profiling is associated with COVID‐19 progression and immune responses

Author

Kevin Ho Wai Yim, Simone Borgoni, and Richard Chahwan

Subjects

clinical liquid biopsy, COVID‐19, diagnosis, extracellular vesicles, SARS‐CoV‐2, Cytology, QH573-671

Abstract

Abstract Coronavirus disease 2019 (COVID‐19) has transformed very quickly into a world pandemic with severe and unexpected consequences on human health. Concerted efforts to generate better diagnostic and prognostic tools have been ongoing. Research, thus far, has primarily focused on the virus itself or the direct immune response to it. Here, we propose extracellular vesicles (EVs) from serum liquid biopsies as a new and unique modality to unify diagnostic and prognostic tools for COVID‐19 analyses. EVs are a novel player in intercellular signalling particularly influencing immune responses. We herein show that innate and adaptive immune EVs profiling, together with SARS‐CoV‐2 Spike S1+ EVs provide a novel signature for SARS‐CoV‐2 infection. It also provides a unique ability to associate the co‐existence of viral and host cell signatures to monitor affected tissues and severity of the disease progression. And provide a phenotypic insight into COVID‐associated EVs.

Published

2022

6. Integrative OMICS Data-Driven Procedure Using a Derivatized Meta-Analysis Approach

Author

Karla Cervantes-Gracia, Richard Chahwan, and Holger Husi

Subjects

meta-analysis, omics, bioinformatics, biomarker analysis, pathway analysis, data integration, Genetics, QH426-470

Abstract

The wealth of high-throughput data has opened up new opportunities to analyze and describe biological processes at higher resolution, ultimately leading to a significant acceleration of scientific output using high-throughput data from the different omics layers and the generation of databases to store and report raw datasets. The great variability among the techniques and the heterogeneous methodologies used to produce this data have placed meta-analysis methods as one of the approaches of choice to correlate the resultant large-scale datasets from different research groups. Through multi-study meta-analyses, it is possible to generate results with greater statistical power compared to individual analyses. Gene signatures, biomarkers and pathways that provide new insights of a phenotype of interest have been identified by the analysis of large-scale datasets in several fields of science. However, despite all the efforts, a standardized regulation to report large-scale data and to identify the molecular targets and signaling networks is still lacking. Integrative analyses have also been introduced as complementation and augmentation for meta-analysis methodologies to generate novel hypotheses. Currently, there is no universal method established and the different methods available follow different purposes. Herein we describe a new unifying, scalable and straightforward methodology to meta-analyze different omics outputs, but also to integrate the significant outcomes into novel pathways describing biological processes of interest. The significance of using proper molecular identifiers is highlighted as well as the potential to further correlate molecules from different regulatory levels. To show the methodology’s potential, a set of transcriptomic datasets are meta-analyzed as an example.

Published

2022

7. Measuring Real-time DNA/RNA Nuclease Activity through Fluorescence

Author

Paulina Wyrzykowska, Sally Rogers, and Richard Chahwan

Subjects

Biology (General), QH301-705.5

Abstract

DNA and RNA nucleases are wide-ranging enzymes, taking part in broad cellular processes from DNA repair to immune response control. Growing interest in the mechanisms and activities of newly discovered nucleases inspired us to share the detailed protocol of our nuclease assay (Sheppard et al., 2019). This easy and inexpensive method can provide data that enables understanding of the molecular mechanism for novel or tested nucleases, from substrate preference and cofactors involved to catalytic rate of reaction.

Published

2021

8. Editorial: Probing the Chromatin Architecture

Author

Francesca Palombo, Stefano Pagliara, Ankur Singh, and Richard Chahwan

Subjects

chromatin organization, cell phenotyping, genome, cancer therapy, vibrational spectroscopy, imaging, Biology (General), QH301-705.5

Published

2021

9. Single Cell Label-Free Probing of Chromatin Dynamics During B Lymphocyte Maturation

Author

Rikke Morrish, Kevin Ho Wai Yim, Stefano Pagliara, Francesca Palombo, Richard Chahwan, and Nicholas Stone

Subjects

B cell, auxeticity, nuclear architecture, chromatin, vibrational spectroscopy, microfluidics, Biology (General), QH301-705.5

Abstract

Large-scale intracellular signaling during developmental growth or in response to environmental alterations are largely orchestrated by chromatin within the cell nuclei. Chemical and conformational modifications of the chromatin architecture are critical steps in the regulation of differential gene expression and ultimately cell fate determination. Therefore, establishing chemical properties of the nucleus could provide key markers for phenotypic characterization of cellular processes on a scale of individual cells. Raman microscopy is a sensitive technique that is capable of probing single cell chemical composition—and sub-cellular regions—in a label-free optical manner. As such, it has great potential in both clinical and basic research. However, perceived limitations of Raman spectroscopy such as low signal intensity and the difficulty in linking alterations in vibrational signals directly with ensuing biological effects have hampered advances in the field. Here we use immune B lymphocyte development as a model to assess chromatin and transcriptional changes using confocal Raman microscopy in combination with microfluidic devices and correlative transcriptomics, thereby linking changes in chemical and structural properties to biological outcomes. Live B lymphocytes were assessed before and after maturation. Multivariate analysis was applied to distinguish cellular components within each cell. The spectral differences between non-activated and activated B lymphocytes were then identified, and their correlation with known intracellular biological changes were assessed in comparison to conventional RNA-seq analysis. Our data shows that spectral analysis provides a powerful tool to study gene activation that can complement conventional molecular biology techniques and opens the way for mapping the dynamics in the biochemical makeup of individual cells.

Published

2021

10. Single Cell Imaging of Nuclear Architecture Changes

Author

Rikke Brandstrup Morrish, Michael Hermes, Jeremy Metz, Nicholas Stone, Stefano Pagliara, Richard Chahwan, and Francesca Palombo

Subjects

B cell, auxeticity, nuclear architecture, chromatin, infrared microscopy, microfluidics, Biology (General), QH301-705.5

Abstract

The dynamic architecture of chromatin, the macromolecular complex comprised primarily of DNA and histones, is vital for eukaryotic cell growth. Chemical and conformational changes to chromatin are important markers of functional and developmental processes in cells. However, chromatin architecture regulation has not yet been fully elucidated. Therefore, novel approaches to assessing chromatin changes at the single-cell level are required. Here we report the use of FTIR imaging and microfluidic cell-stretcher chips to assess changes to chromatin architecture and its effect on the mechanical properties of the nucleus in immune cells. FTIR imaging enables label-free chemical imaging with subcellular resolution. By optimizing the FTIR methodology and coupling it with cell segmentation analysis approach, we have identified key spectral changes corresponding to changes in DNA levels and chromatin conformation at the single cell level. By further manipulating live single cells using pressure-driven microfluidics, we found that chromatin decondensation – either during general transcriptional activation or during specific immune cell maturation – can ultimately lead to nuclear auxeticity which is a new biological phenomenon recently identified. Taken together our findings demonstrate the tight and, potentially bilateral, link between extra-cellular mechanotransduction and intra-cellular nuclear architecture.

Published

2019

11. Epigenomic Modifications Mediating Antibody Maturation

Author

Emily C. Sheppard, Rikke Brandstrup Morrish, Michael J. Dillon, Rebecca Leyland, and Richard Chahwan

Subjects

epigenetic modifications, epigenomics and epigenetics, antibody diversity, cytosine deamination, somatic hypermutation, class-switch recombination, Immunologic diseases. Allergy, RC581-607

Abstract

Epigenetic modifications, such as histone modifications, DNA methylation status, and non-coding RNAs (ncRNA), all contribute to antibody maturation during somatic hypermutation (SHM) and class-switch recombination (CSR). Histone modifications alter the chromatin landscape and, together with DNA primary and tertiary structures, they help recruit Activation-Induced Cytidine Deaminase (AID) to the immunoglobulin (Ig) locus. AID is a potent DNA mutator, which catalyzes cytosine-to-uracil deamination on single-stranded DNA to create U:G mismatches. It has been shown that alternate chromatin modifications, in concert with ncRNAs and potentially DNA methylation, regulate AID recruitment and stabilize DNA repair factors. We, hereby, assess the combination of these distinct modifications and discuss how they contribute to initiating differential DNA repair pathways at the Ig locus, which ultimately leads to enhanced antibody–antigen binding affinity (SHM) or antibody isotype switching (CSR). We will also highlight how misregulation of epigenomic regulation during DNA repair can compromise antibody development and lead to a number of immunological syndromes and cancer.

Published

2018

12. Review for 'Z‐nucleic acids: uncovering the functions from past to present'

Author

Richard Chahwan

Published

2022

13. Assessing extracellular vesicles in human biofluids using flow-based analyzers

Author

Olga Krzyzaniak, Kevin Ho Wai Yim, Ala’a Al Hrout, Ben Peacock, Richard Chahwan, and University of Zurich

Subjects

570 Life sciences, biology, 610 Medicine & health, 10263 Institute of Experimental Immunology, UFSP13-5 Translational Cancer Research

Abstract

Extracellular vesicles (EVs) are increasingly being analyzed by flow cytometry. Yet, their miniscule size and low refractive index, causes the scatter intensity of most EVs to fall below the detection limit of most flow cytometers. A new class of devices, known as spectral flow analyzers, are becoming standards in cell phenotyping studies. Largely, due to their unique capacity of detecting a vast panel of markers with higher sensitivity for light scatter detection. Another class of devices, known as nano-analyzers, provides high resolution detection of sub-micron sized particles. Here, we aim to compare the EVs phenotyping performance between the Aurora (Cytek) spectral cell analyzer and the NanoFCM (nFCM) nanoflow analyzer. These two devices were specifically chosen given their lead in becoming gold standards in their respective fields. Immune cell-derived EVs remain poorly characterized despite their clinical potentials. We therefore, used B- and T- cell line-derived EVs and donor-matched human biofluid-derived EVs from serum, urine, and saliva in combination with a panel of established immune markers for this comparative study. A comparative evaluation of both cytometry platforms was performed, discussing their potential and suitability for different applications. We found that nFCM can accurately i) analyze small EVs (40 to 200 nm) matching the size accuracy of electron microscopy; ii) measure concentration of single EV particle per volume; iii) identify underrepresented EV marker subsets; and iv) provide co-localization of EV surface markers. We could also show that human sample biofluids have unique EV marker signatures that could have future clinical relevance.

Published

2022

14. Role of EXO1 nuclease activity in genome maintenance, the immune response and tumor suppression in Exo1D173A mice

Author

Shanzhi, Wang, Kyeryoung, Lee, Stephen, Gray, Yongwei, Zhang, Catherine, Tang, Rikke B, Morrish, Elena, Tosti, Johanna, van Oers, Mohammad Ruhul, Amin, Paula E, Cohen, Thomas, MacCarthy, Sergio, Roa, Matthew D, Scharff, Winfried, Edelmann, and Richard, Chahwan

Subjects

B-Lymphocytes, Meiosis, Mice, DNA Repair Enzymes, Exodeoxyribonucleases, DNA Repair, Neoplasms, Immunity, Animals, Somatic Hypermutation, Immunoglobulin

Abstract

DNA damage response pathways rely extensively on nuclease activity to process DNA intermediates. Exonuclease 1 (EXO1) is a pleiotropic evolutionary conserved DNA exonuclease involved in various DNA repair pathways, replication, antibody diversification, and meiosis. But, whether EXO1 facilitates these DNA metabolic processes through its enzymatic or scaffolding functions remains unclear. Here, we dissect the contribution of EXO1 enzymatic versus scaffolding activity by comparing Exo1DA/DA mice expressing a proven nuclease-dead mutant form of EXO1 to entirely EXO1-deficient Exo1-/- and EXO1 wild type Exo1+/+ mice. We show that Exo1DA/DA and Exo1-/- mice are compromised in canonical DNA repair processing, suggesting that the EXO1 enzymatic role is important for error-free DNA mismatch and double-strand break repair pathways. However, in non-canonical repair pathways, EXO1 appears to have a more nuanced function. Next-generation sequencing of heavy chain V region in B cells showed the mutation spectra of Exo1DA/DA mice to be intermediate between Exo1+/+ and Exo1-/- mice, suggesting that both catalytic and scaffolding roles of EXO1 are important for somatic hypermutation. Similarly, while overall class switch recombination in Exo1DA/DA and Exo1-/- mice was comparably defective, switch junction analysis suggests that EXO1 might fulfill an additional scaffolding function downstream of class switching. In contrast to Exo1-/- mice that are infertile, meiosis progressed normally in Exo1DA/DA and Exo1+/+ cohorts, indicating that a structural but not the nuclease function of EXO1 is critical for meiosis. However, both Exo1DA/DA and Exo1-/- mice displayed similar mortality and cancer predisposition profiles. Taken together, these data demonstrate that EXO1 has both scaffolding and enzymatic functions in distinct DNA repair processes and suggest a more composite and intricate role for EXO1 in DNA metabolic processes and disease.

Published

2022

15. Predictive and Prognostic Value of Non-Coding RNA in Breast Cancer

Author

Navid Sobhani, Richard Chahwan, Raheleh Roudi, Rachel Morris, Stefano Volinia, Dafei Chai, Alberto D’Angelo, Daniele Generali, University of Zurich, and Sobhani, Navid

Subjects

Cancer Research, Oncology, 570 Life sciences, biology, 610 Medicine & health, 2730 Oncology, 1306 Cancer Research, 10263 Institute of Experimental Immunology, oncology_oncogenics, UFSP13-5 Translational Cancer Research

Abstract

For decades since the central dogma, cancer biology research has been focusing on the involvement of genes encoding proteins. It has been not until more recent times that a new molecular class has been discovered, named non-coding RNA (ncRNA), which has been shown to play crucial roles in shaping the activity of cells. An extraordinary number of studies into shown that ncRNAs represent an extensive and prevalent group of RNAs, including both oncogenic or tumor suppressive molecules. Henceforth, various clinical trials involving ncRNAs as extra ordinary biomarkers or therapies have started to emerge. In this review, we will focus on the prognostic and diagnostic role of ncRNAs for breast cancer.

Published

2022

16. Serum extracellular vesicles trace COVID-19 progression and immune responses

Author

Kevin Ho Wai Yim, Simone Borgoni, and Richard Chahwan

Abstract

Coronavirus disease 2019 (COVID-19) has transformed very quickly into a world pandemic with severe and unexpected consequences on human health. Concerted efforts to generate better diagnostic and prognostic tools have been ongoing. Research, thus far, has primarily focused on the virus itself or the direct immune response to it. Here, we propose extracellular vesicles (EVs) from serum liquid biopsies as a new and unique modality to unify diagnostic and prognostic tools for COVID-19 analyses. EVs are a novel player in intercellular signaling particularly influencing immune responses. We herein show that innate and adaptive immune EVs profiling, together with SARS-CoV-2 Spike S1+ EVs provide a novel signature for COVID-19 infection. It also provides a unique ability to trace the co-existence of viral and host cell signatures to monitor affected tissues and severity of the disease progression. And provide a phenotypic insight into COVID-associated EVs.

Published

2022

17. Integrative OMICS Data-Driven Procedure Using a Derivatized Meta-Analysis Approach

Author

Karla, Cervantes-Gracia, Richard, Chahwan, and Holger, Husi

Abstract

The wealth of high-throughput data has opened up new opportunities to analyze and describe biological processes at higher resolution, ultimately leading to a significant acceleration of scientific output using high-throughput data from the different omics layers and the generation of databases to store and report raw datasets. The great variability among the techniques and the heterogeneous methodologies used to produce this data have placed meta-analysis methods as one of the approaches of choice to correlate the resultant large-scale datasets from different research groups. Through multi-study meta-analyses, it is possible to generate results with greater statistical power compared to individual analyses. Gene signatures, biomarkers and pathways that provide new insights of a phenotype of interest have been identified by the analysis of large-scale datasets in several fields of science. However, despite all the efforts, a standardized regulation to report large-scale data and to identify the molecular targets and signaling networks is still lacking. Integrative analyses have also been introduced as complementation and augmentation for meta-analysis methodologies to generate novel hypotheses. Currently, there is no universal method established and the different methods available follow different purposes. Herein we describe a new unifying, scalable and straightforward methodology to meta-analyze different omics outputs, but also to integrate the significant outcomes into novel pathways describing biological processes of interest. The significance of using proper molecular identifiers is highlighted as well as the potential to further correlate molecules from different regulatory levels. To show the methodology's potential, a set of transcriptomic datasets are meta-analyzed as an example.

Published

2021

18. Modelling liver cancer microenvironment: novel 3D culture system as a potential anti-cancer drug screening tool

Author

Richard Chahwan, Amr Amin, Ala’a Al Hrout, and Karla Cervantes-Gracia

Subjects

Tumor microenvironment, In vivo, Hepatocellular carcinoma, Cancer cell, medicine, Cancer research, Biology, Carcinogenesis, medicine.disease_cause, medicine.disease, Liver cancer, Ex vivo, Metastasis

Abstract

The tumor microenvironment and its contribution to tumorigenesis has been a focal highlight in recent years. A two-way communication between the tumor and the surrounding microenvironment sustains and contributes to the growth and metastasis of tumors. Progression and metastasis of hepatocellular carcinoma have been reported to be exceedingly influenced by diverse microenvironmental cues. In this study, we present a 3D-culture model of liver cancer to better mimic in vivo tumor settings. By creating novel 3D co-culture model that combines free-floating and scaffold based 3D-culture techniques of liver cancer cells and fibroblasts, we aimed to establish a simple albeit reproducible ex vivo cancer microenvironment model that captures tumor-stroma interactions. The model presented herein exhibited unique gene expression and protein expression profiles when compared to 2D and 3D mono-cultures of liver cancer cells. Our results showed that in vivo like conditions cannot be mimicked by simply growing cancer cells as spheroids, but by co-culturing them with 3D fibroblast with which they were able to cross-talk. This was evident by the upregulation of several pathways involved in HCC, and the increase in secreted factors by co-cultured cancer cells, many of which are also involved in tumor-stroma interactions. Compared to the conventional 2D culture, the proposed model exhibits an increase in the expression of genes associated with development, progression, and poor prognosis of HCC. Our results correlated with an aggressive outcome that better mirrors in vivo HCC, and therefore, a more reliable platform for molecular understanding of HCC and possibly better anti-cancer drug screening.

Published

2021

19. Role of EXO1 nuclease activity in genome maintenance, the immune response and tumor suppression in Exo1D173A mice

Author

Richard Chahwan, Stephen Gray, Sergio Roa, Shanzhi Wang, Thomas MacCarthy, Matthew D. Scharff, Winfried Edelmann, Yongwei Zhang, Rikke Morrish, Catherine Tangcatherin, Kyeryoung Lee, Elena Tosti, Johanna van Oers, and Paula E. Cohen

Subjects

Nuclease, chemistry.chemical_compound, Exonuclease 1, biology, Chemistry, DNA repair, DNA damage, Mutant, biology.protein, Somatic hypermutation, DNA Exonuclease, DNA, Cell biology

Abstract

DNA damage response pathways rely extensively on nuclease activity to process DNA intermediates. Exonuclease 1 (EXO1) is a pleiotropic evolutionary conserved DNA exonuclease involved in various DNA repair pathways, replication, antibody diversification, and meiosis. But, whether EXO1 facilitates these DNA metabolic processes through its enzymatic or scaffolding functions remains unclear. Here we dissect the contribution of EXO1 enzymatic versus scaffolding activity by comparing Exo1DA/DA mice expressing a proven nuclease-dead mutant form of EXO1 to entirely EXO1-deficient Exo1−/− and EXO1 wild type Exo1+/+ mice. We show that Exo1DA/DA and Exo1−/− mice are compromised in canonical DNA repair processing, suggesting that the EXO1 enzymatic role is important for error-free DNA mismatch and double-strand break repair pathways. However, in non-canonical repair pathways, EXO1 appears to have a more nuanced function. Next-generation sequencing of heavy chain V region in B cells showed the mutation spectra of Exo1DA/DA mice to be intermediate between Exo1+/+ and Exo1−/− mice, suggesting that both catalytic and scaffolding roles of EXO1 are important for somatic hypermutation. Similarly, while overall class switch recombination in Exo1DA/DA and Exo1−/− mice was comparably defective, switch-switch junction analysis suggests that EXO1 might fulfill an additional scaffolding function downstream of class switching. In contrast to Exo1−/− mice that are infertile, meiosis progressed normally in Exo1DA/DA and Exo1+/+ cohorts, indicating that a structural but not the nuclease function of EXO1 is critical for meiosis. However, both Exo1DA/DA and Exo1−/− mice displayed similar mortality and cancer predisposition profiles. Taken together, these data demonstrate that EXO1 has both scaffolding and enzymatic functions in distinct DNA repair processes and suggest a more composite and intricate role for EXO1 in DNA metabolic processes and disease.

Published

2021

20. Integrative Analysis of Incongruous Cancer Genomics and Proteomics Datasets

Author

Karla, Cervantes-Gracia, Richard, Chahwan, and Holger, Husi

Subjects

Proteomics, Neoplasms, Systems Biology, Humans, Genomics, Biomarkers

Abstract

Cancer is a complex disease characterized by molecular heterogeneity and the involvement of several cellular mechanisms throughout its evolution and pathogenesis. Despite the great efforts made to untangle these mechanisms, cancer pathophysiology remains far from clear. So far, panels of biomarkers have been reported from high-throughput data generated through different platforms. These biomarkers are primarily focused on one type of coding molecules such as transcripts or proteins, mainly due to the apparent heterogeneity of output data resulting from the use of various techniques specific to the molecular type. Hence, there is a major need to understand how these molecules interact and complement each other to be able to explain the deregulated processes involved. The breadth of large-scale data availability as well as the lack of in-depth analysis of publicly available data has raised concerns and enabled opportunities for new strategies to analyze "Big data" more comprehensively. Here, a new protocol to perform integrative analysis based on a systems biology approach is described. The foundation of the approach relies on groups of datasets from published studies compared within the original described groups and organized in a designated format to allow the integration and cross-comparison among different studies and different platforms. This approach follows an unbiased hypothesis-free methodology that will facilitate the identification of commonalities among different data-set sources, and ultimately map and characterize specific molecular pathways using significantly deregulated molecules. This in turn will generate novel insights about the mechanisms deregulated in complex diseases such as cancer.

Published

2021

21. APOBECs orchestrate genomic and epigenomic editing across health and disease

Author

Richard Chahwan, Anna Gramalla-Schmitz, Julian Weischedel, Karla Cervantes-Gracia, University of Zurich, and Chahwan, Richard

Subjects

APOBEC, Epigenomics, Genome, Retroelements, DNA damage, RNA, 610 Medicine & health, Computational biology, Genomics, Biology, 10263 Institute of Experimental Immunology, chemistry.chemical_compound, DNA demethylation, 1311 Genetics, chemistry, Cytidine Deaminase, Genetics, Nucleic acid, 570 Life sciences, biology, APOBEC Deaminases, DNA, Tissue homeostasis

Abstract

APOBEC proteins can deaminate cytosine residues in DNA and RNA. This can lead to somatic mutations, DNA breaks, RNA modifications, or DNA demethylation in a selective manner. APOBECs function in various cellular compartments and recognize different nucleic acid motifs and structures. They orchestrate a wide array of genomic and epigenomic modifications, thereby affecting various cellular functions positively or negatively, including immune editing, viral and retroelement restriction, DNA damage responses, DNA demethylation, gene expression, and tissue homeostasis. Furthermore, the cumulative increase in genomic and epigenomic editing with aging could also, at least in part, be attributed to APOBEC function. We synthesize our cumulative understanding of APOBEC activity in a unifying overview and discuss their genomic and epigenomic impact in physiological, pathological, and technological contexts.

Published

2021

22. Integrative Analysis of Incongruous Cancer Genomics and Proteomics Datasets

Author

Richard Chahwan, Holger Husi, and Karla Cervantes-Gracia

Subjects

business.industry, Computer science, Molecular type, Systems biology, Big data, Complex disease, Cancer, Genomics, Computational biology, medicine.disease, Proteomics, medicine, Identification (biology), business

Abstract

Cancer is a complex disease characterized by molecular heterogeneity and the involvement of several cellular mechanisms throughout its evolution and pathogenesis. Despite the great efforts made to untangle these mechanisms, cancer pathophysiology remains far from clear. So far, panels of biomarkers have been reported from high-throughput data generated through different platforms. These biomarkers are primarily focused on one type of coding molecules such as transcripts or proteins, mainly due to the apparent heterogeneity of output data resulting from the use of various techniques specific to the molecular type. Hence, there is a major need to understand how these molecules interact and complement each other to be able to explain the deregulated processes involved. The breadth of large-scale data availability as well as the lack of in-depth analysis of publicly available data has raised concerns and enabled opportunities for new strategies to analyze "Big data" more comprehensively. Here, a new protocol to perform integrative analysis based on a systems biology approach is described. The foundation of the approach relies on groups of datasets from published studies compared within the original described groups and organized in a designated format to allow the integration and cross-comparison among different studies and different platforms. This approach follows an unbiased hypothesis-free methodology that will facilitate the identification of commonalities among different data-set sources, and ultimately map and characterize specific molecular pathways using significantly deregulated molecules. This in turn will generate novel insights about the mechanisms deregulated in complex diseases such as cancer.

Published

2021

23. Measuring Real-time DNA/RNA Nuclease Activity through Fluorescence

Author

Sally L. Rogers, Paulina Wyrzykowska, Richard Chahwan, University of Zurich, and Chahwan, Richard

Subjects

DNA repair, Strategy and Management, 610 Medicine & health, 10263 Institute of Experimental Immunology, Industrial and Manufacturing Engineering, Cofactor, chemistry.chemical_compound, 1300 General Biochemistry, Genetics and Molecular Biology, 2400 General Immunology and Microbiology, 1110 Plant Science, Methods Article, Ribonuclease, UFSP13-5 Translational Cancer Research, chemistry.chemical_classification, Nuclease, biology, Mechanical Engineering, Metals and Alloys, 2800 General Neuroscience, RNA, Fluorescence, Enzyme, Biochemistry, chemistry, biology.protein, 570 Life sciences, DNA

Abstract

DNA and RNA nucleases are wide-ranging enzymes, taking part in broad cellular processes from DNA repair to immune response control. Growing interest in the mechanisms and activities of newly discovered nucleases inspired us to share the detailed protocol of our nuclease assay ( Sheppard et al., 2019 ). This easy and inexpensive method can provide data that enables understanding of the molecular mechanism for novel or tested nucleases, from substrate preference and cofactors involved to catalytic rate of reaction.

Published

2021

24. Extracellular Vesicles Orchestrate Immune and Tumor Interaction Networks

Author

Ala’a Al Hrout, Richard Chahwan, Kevin Ho Wai Yim, Simone Borgoni, University of Zurich, and Chahwan, Richard

Subjects

0301 basic medicine, Cancer Research, non-coding RNA, 610 Medicine & health, Review, Biology, 10263 Institute of Experimental Immunology, Extracellular vesicles, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immune system, Exponential growth, tumor microenvironment, 1306 Cancer Research, Epigenomics, Tumor microenvironment, Non-coding RNA, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell biology, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Nucleic acid, 570 Life sciences, biology, immune signaling, 2730 Oncology, extracellular vesicles, Intracellular

Abstract

Simple Summary Significant strides have been made to describe the pervasive role of extracellular vesicles (EVs) in health and disease. This work provides an insightful and unifying mechanistic understanding of EVs in immunity and tumorigenesis. This is achieved by dissecting the role of EVs within the continuum of immune cell physiology, immune–infection responses, and the immune–tumor microenvironment. Our work synthesizes important topical findings on immune EV signaling in mediating immune–tumor interaction networks. Abstract Extracellular vesicles (EVs) are emerging as potent and intricate intercellular communication networks. From their first discovery almost forty years ago, several studies have bolstered our understanding of these nano-vesicular structures. EV subpopulations are now characterized by differences in size, surface markers, cargo, and biological effects. Studies have highlighted the importance of EVs in biology and intercellular communication, particularly during immune and tumor interactions. These responses can be equally mediated at the proteomic and epigenomic levels through surface markers or nucleic acid cargo signaling, respectively. Following the exponential growth of EV studies in recent years, we herein synthesize new aspects of the emerging immune–tumor EV-based intercellular communications. We also discuss the potential role of EVs in fundamental immunological processes under physiological conditions, viral infections, and tumorigenic conditions. Finally, we provide insights on the future prospects of immune–tumor EVs and suggest potential avenues for the use of EVs in diagnostics and therapeutics.

Published

2020

25. Oxidative stress and inflammation in the development of cardiovascular disease and contrast induced nephropathy

Author

Daniel Llanas-Cornejo, Richard Chahwan, Khuram Raja, Ian L. Megson, James N. Cobley, Holger Husi, and Karla Cervantes-Gracia

Subjects

chemistry.chemical_classification, Reactive oxygen species, business.industry, Contrast-induced nephropathy, Inflammation, Disease, medicine.disease, medicine.disease_cause, chemistry, Immunology, medicine, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Oxidative stress

Published

2020

26. Functional Phenotype Flow Cytometry: On Chip Sorting of Individual Cells According to Responses to Stimuli

Author

Petar O. Nikiforov, Richard Chahwan, Beata Hejja, Fabrice Gielen, Christian Soeller, Catalin Chimerel, University of Zurich, and Chimerel, Catalin

Subjects

medicine.drug_class, Microfluidics, Biomedical Engineering, 2204 Biomedical Engineering, Receptors, Antigen, B-Cell, 610 Medicine & health, 2700 General Medicine, Stimulus (physiology), 10263 Institute of Experimental Immunology, Monoclonal antibody, General Biochemistry, Genetics and Molecular Biology, Cell Line, Flow cytometry, Biomaterials, 03 medical and health sciences, 1300 General Biochemistry, Genetics and Molecular Biology, medicine, Humans, 030304 developmental biology, 0303 health sciences, medicine.diagnostic_test, Chemistry, 2502 Biomaterials, 030302 biochemistry & molecular biology, breakpoint cluster region, Cell sorting, Flow Cytometry, Phenotype, Cell biology, Cancer cell, 570 Life sciences, biology, Intracellular

Abstract

The ability to effectively separate and isolate biological cells into specific and well-defined subpopulations is crucial for the advancement of our understanding of cellular heterogeneity and its relevance to living systems. Here is described the development of the functional phenotype flow cytometer (FPFC), a new device designed to separate cells on the basis of their in situ real-time phenotypic responses to stimuli. The FPFC performs a cascade of cell processing steps on a microfluidic platform: introduces biological cells one at a time into a solution of a biological reagent that acts as a stimulus, incubates the cells with the stimulus solution in a flow, and sorts the cells into subpopulations according to their phenotypic responses to the provided stimulus. The presented implementation of the FPFC uses intracellular fluorescence as a readout, incubates cells for 75 s, and operates at a throughput of up to 4 cells min$^{-1}$ -resulting in the profiling and sorting of hundreds of cells within a few hours. The design and operation of the FPFC are validated by sorting cells from the human Burkitt's lymphoma cancerous cell line Ramos on the basis of their response to activation of the B cell antigen receptor (BCR) by a targeted monoclonal antibody.

Published

2021

27. A universal fluorescence-based toolkit for real-time quantification of DNA and RNA nuclease activity

Author

Emily C. Sheppard, Richard Chahwan, Nicholas J. Harmer, Sally L. Rogers, University of Zurich, and Chahwan, Richard

Subjects

0301 basic medicine, DNA Repair, DNA polymerase, DNA repair, DNA, Single-Stranded, lcsh:Medicine, 610 Medicine & health, DNA-Directed DNA Polymerase, 10263 Institute of Experimental Immunology, Biochemical assays, Article, Fluorescence, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, Ribonucleases, 0302 clinical medicine, Humans, Directionality, Ribonuclease, lcsh:Science, Enzyme Assays, 030304 developmental biology, 1000 Multidisciplinary, 0303 health sciences, Nuclease, Deoxyribonucleases, Multidisciplinary, biology, Chemistry, lcsh:R, 030302 biochemistry & molecular biology, RNA, Phosphoproteins, 3. Good health, Kinetics, Exodeoxyribonucleases, 030104 developmental biology, Biochemistry, Enzyme mechanisms, DNA methylation, biology.protein, 570 Life sciences, lcsh:Q, 030217 neurology & neurosurgery, DNA

Abstract

DNA and RNA nucleases play a critical role in a growing number of cellular processes ranging from DNA repair to immune surveillance. Nevertheless, many nucleases have unknown or poorly characterized activities. Elucidating nuclease substrate specificities and regulatory components can support a more definitive understanding of cellular mechanisms in physiology and disease. Using fluorescence-based methods, we have developed a quick, safe, reproducible, cost-effective, and real-time nuclease assay toolkit that could be used for small- and large- scale experimental assays. Additionally, these data can be analysed to determine each reaction's unique enzyme kinetics. We have designed a library of substrates that can be used to study catalytic rates, directionality, and substrate preferences. The assay is sensitive enough to detect kinetics of repair enzymes when confronted with DNA mismatches or DNA methylation sites. We have also extended this assay to consider analysing the kinetics of human single-strand DNA nuclease TREX2, DNA polymerases, and RNA:DNA nucleases, which are also involved in DNA repair and immune regulation, and have been associated with various disease conditions, including cancer and immune disorders.

Published

2019

28. The MutSβ complex is a modulator of p53-driven tumorigenesis through its functions in both DNA double-strand break repair and mismatch repair

Author

Ximo Pechuan, Yarong Wang, Richard Chahwan, Y Edwards, Weijia Zhang, Aviv Bergman, Winfried Edelmann, Cameron Smith, Matthew D. Scharff, J M M van Oers, Bo Jin, Sonja Schaetzlein, University of Zurich, and Edelmann, W

Subjects

Cancer Research, DNA Copy Number Variations, Carcinogenesis, Loss of Heterozygosity, 610 Medicine & health, Biology, 10263 Institute of Experimental Immunology, medicine.disease_cause, DNA Mismatch Repair, Article, Mice, 1311 Genetics, Chromosomal Instability, Chromosome instability, 1312 Molecular Biology, Genetics, medicine, Animals, 1306 Cancer Research, DNA Breaks, Double-Stranded, Molecular Biology, Cells, Cultured, Mice, Knockout, Proteins, Microsatellite instability, Sarcoma, medicine.disease, Double Strand Break Repair, Mice, Inbred C57BL, MSH3, Tumor progression, MSH2, MutS Homolog 3 Protein, Cancer research, 570 Life sciences, biology, DNA mismatch repair, Tumor Suppressor Protein p53

Abstract

Loss of the DNA mismatch repair protein MSH3 leads to the development of a variety of tumors in mice without significantly affecting survival rates, suggesting a modulating role for the MutSβ (MSH2-MSH3) complex in late onset tumorigenesis. To better study the role of MSH3 in tumor progression, we crossed Msh3−/− mice onto a tumor predisposing p53-deficient background. Survival of Msh3/p53 mice was not reduced compared to single p53 mutant mice; however, the tumor spectrum changed significantly from lymphoma to sarcoma, indicating MSH3 as a potent modulator of p53-driven tumorigenesis. Interestingly, Msh3−/− mouse embryonic fibroblasts displayed increased chromatid breaks and persistence of γH2AX foci following ionizing radiation, indicating a defect in DNA double strand break repair. Msh3/p53 tumors showed increased loss of heterozygosity, elevated genome-wide copy number variation, and a moderate microsatellite instability phenotype compared to Msh2/p53 tumors, revealing that MSH2-MSH3 suppresses tumorigenesis by maintaining chromosomal stability. Our results show that the MSH2-MSH3 complex is important for the suppression of late onset tumors due to its role in DNA double strand break repair as well as in DNA mismatch repair. Furthermore, they demonstrate that MSH2-MSH3 suppresses chromosomal instability and modulates the tumor spectrum in p53-deficient tumorigenesis, and possibly plays a role in other chromosomally unstable tumors as well.

Published

2013

29. Dma/RNF8 proteins are evolutionarily conserved E3 ubiquitin ligases that target septins

Author

Serge Gravel, Stephen P. Jackson, Richard Chahwan, Takahiro Matsusaka, University of Zurich, and Chahwan, Richard

Subjects

Saccharomyces cerevisiae Proteins, 610 Medicine & health, cytokinesis, Cell Cycle Proteins, 10263 Institute of Experimental Immunology, Septin, RNF8, 1309 Developmental Biology, 1307 Cell Biology, Dma1, 03 medical and health sciences, Dma2, Ubiquitin, Report, CHFR, ubiquitin, Schizosaccharomyces, 1312 Molecular Biology, septins, Humans, Cell Cycle Protein, Molecular Biology, 030304 developmental biology, 0303 health sciences, septin-ring, biology, 030302 biochemistry & molecular biology, Ubiquitin-Protein Ligases, Chfr, Cell Biology, 3. Good health, Ubiquitin ligase, Cell biology, DNA-Binding Proteins, Septin ring, E3 ubiquitin ligase, midbody, biology.protein, 570 Life sciences, Schizosaccharomyces pombe Proteins, Cytokinesis, Developmental Biology

Abstract

The budding yeast proteins Dma1 and Dma2 are members of the unique FHA-RING domain protein family and are linked to mitotic regulation and septin organization by ill-defined mechanisms. We show that Dma2 has ubiquitin ligase activity, and that septins Shs1 and Cdc11 are likely direct in vivo targets. We further propose that human RNF8, rather than Chfr, is the mammalian Dma homolog. As in yeast, RNF8 localizes to the centrosomes and cell division sites and promotes ubiquitylation of the septin SEPT7, whose depletion increases cell division anomalies. Together, these findings reveal evolutionary and functional conservation of Dma proteins, and suggest that RNF8 maintains genome stability through independent, yet analogous, nuclear and cytoplasmic ubiquitylation activities.

Published

2013

30. Isotype switching: Mouse IgG3 constant region drives increased affinity for polysaccharide antigens

Author

Richard Chahwan, Nicholas J. Harmer, University of Zurich, and Harmer, Nicholas J

Subjects

0301 basic medicine, Burkholderia pseudomallei, Antibody Affinity, 2405 Parasitology, Receptors, Fc, 10263 Institute of Experimental Immunology, 2726 Microbiology (medical), Mice, chemistry.chemical_classification, Constant region, isotype switching, Immunogenicity, 2404 Microbiology, Antibodies, Monoclonal, food and beverages, Vaccination, Editorial, Infectious Diseases, Protein Binding, Research Paper, Microbiology (medical), 030106 microbiology, Immunology, chemical and pharmacologic phenomena, 610 Medicine & health, Biology, Polysaccharide, complex mixtures, Microbiology, 03 medical and health sciences, Immune system, Antigen, Polysaccharides, antibody multimerization, Animals, Bacterial Capsules, 2403 Immunology, IgG3, 2725 Infectious Diseases, vaccination, biology.organism_classification, Immunoglobulin Class Switching, 030104 developmental biology, chemistry, Immunoglobulin class switching, polysaccharide, Immunoglobulin G, Proteolysis, 570 Life sciences, biology, Parasitology

Abstract

Immunoglobulin G3 (IgG3) is the predominant IgG subclass elicited in response to polysaccharide antigens in mice. This specific subclass has been shown to crosslink its fragment crystallizable (Fc) regions following binding to multivalent polysaccharides. Crosslinking leads to increased affinity through avidity, which theoretically should lead to more effective protection against bacteria and yeast displaying capsular polysaccharides on their surface. To investigate this further we have analyzed the binding characteristics of 2 IgG monoclonal antibody (mAb) subclass families that bind to the capsular polysaccharide (CPS) of Burkholderia pseudomallei. The first subclass family originated from an IgG3 hybridoma cell line (3C5); the second family was generated from an IgG1 cell line (2A5). When the Fc region of the 3C5 IgG3 is removed by proteolytic cleavage, the resulting F(ab')2 fragments exhibit decreased affinity compared to the full-length mAb. Similarly, when the parent IgG3 mAb is subclass-switched to IgG1, IgG2b, and IgG2a, all of these subclasses exhibit decreased affinity. This decrease in affinity is not seen when the 2A5 IgG1 mAb is switched to an IgG2b or IgG2a, strongly suggesting the drop in affinity is related to the IgG3 Fc region.

Published

2016

31. AIDing antibody diversity by error-prone mismatch repair

Author

Richard Chahwan, Sergio Roa, Winfried Edelmann, Matthew D. Scharff, University of Zurich, and Scharff, Matthew D

Subjects

Immunology, Somatic hypermutation, 610 Medicine & health, 10263 Institute of Experimental Immunology, DNA Mismatch Repair, Article, chemistry.chemical_compound, Cytidine Deaminase, Activation-induced (cytidine) deaminase, Animals, Humans, Immunology and Allergy, Gene, Genetics, 2403 Immunology, biology, Ubiquitination, Antibody Diversity, Cytidine deaminase, Immunoglobulin class switching, chemistry, Deamination, Mutation, 2723 Immunology and Allergy, biology.protein, 570 Life sciences, DNA mismatch repair, DNA

Abstract

The creation of a highly diverse antibody repertoire requires the synergistic activity of a DNA mutator, known as activation-induced deaminase (AID), coupled with an error-prone repair process that recognizes the DNA mismatch catalyzed by AID. Instead of facilitating the canonical error-free response, which generally occurs throughout the genome, DNA mismatch repair (MMR) participates in an error-prone repair mode that promotes A:T mutagenesis and double-strand breaks at the immunoglobulin (Ig) genes. As such, MMR is capable of compounding the mutation frequency of AID activity as well as broadening the spectrum of base mutations; thereby increasing the efficiency of antibody maturation. We here review the current understanding of this MMR-mediated process and describe how the MMR signaling cascade downstream of AID diverges in a locus dependent manner and even within the Ig locus itself to differentially promote somatic hypermutation (SHM) and class switch recombination (CSR) in B cells.

Published

2012

32. Aicardi-Goutieres syndrome: from patients to genes and beyond

Author

C Chahwan, Richard Chahwan, University of Zurich, and Chahwan, Charly

Subjects

2716 Genetics (clinical), 610 Medicine & health, Biology, 10263 Institute of Experimental Immunology, Nervous System Malformations, Autoimmune Diseases, Autoimmune Diseases of the Nervous System, Immune system, 1311 Genetics, Metabolic Diseases, Interferon, Genetics, medicine, Animals, Humans, Vascular Diseases, Progressive encephalopathy, Hereditary Neurodegenerative Disorder, Gene, Genetics (clinical), Early onset, Brain Diseases, medicine.disease, Immunology, 570 Life sciences, biology, Aicardi–Goutières syndrome, SAMHD1, medicine.drug

Abstract

Chahwan C, Chahwan R. Aicardi–Goutieres syndrome: from patients to genes and beyond. Aicardi–Goutieres syndrome (AGS) is a hereditary neurodegenerative disorder characterized mainly by early onset progressive encephalopathy, concomitant with an increase in interferon-α levels in the cerebrospinal fluid. Although it was initially mistaken for intrauterine viral infections, AGS has now been genetically attributed to a lack of adequate processing of cellular nucleic acid debris, which culminates in the perpetual trigger of the innate and acquired immune responses. Although the exact mechanisms governing AGS are not fully understood, significant strides have been recently achieved in better characterizing the disorder and the molecular functions of the five known proteins found mutated in AGS. Studies have now uncovered that AGS is tightly linked with the predisposition to other autoimmune disorders such as familial chilblain lupus and systemic lupus erythematosus. Moreover, at least two of the proteins mutated in AGS, namely TREX1 and SAMHD1, also seem to have antagonistic roles in safeguarding humans from human immunodeficiency virus (HIV) infections. We hereby synthesize the current developments into the greater framework of AGS and suggest that a better understanding of AGS might help usher a better treatment not only for some autoimmune disorders but also possibly for patients suffering from HIV infections, too.

Published

2012

33. Error-Prone Mismatch and Base Excision DNA Repair in Somatic Hypermutation

Author

Matthew D. Scharff, Richard Chahwan, Lirong Wei, Shanzhi Wang, University of Zurich, Ratcliffe, M J H, and Wang, Shanzhi

Subjects

Genetics, Somatic cell, DNA repair, Germinal center, Somatic hypermutation, 610 Medicine & health, 2700 General Medicine, Base excision repair, Biology, 10263 Institute of Experimental Immunology, Immunoglobulin class switching, 570 Life sciences, biology, DNA mismatch repair, Nucleotide excision repair

Abstract

The large repertoire of antibodies that is achieved through V(D)J recombination does not create antibodies that have sufficient affinity and broad enough specificity to protect against all toxins and pathogenic organisms. To create such antibodies, B cells somatically hypermutate the antibody variable regions to increase affinity and the Ig switch regions to express those mutated variable regions with each of the isotypes through class switch recombination. This article focuses on how somatic mutations generated by activation-induced deaminase in the variable and switch regions are extended by noncanonical error-prone mismatch and base excision repair.

Published

2016

34. Eme1 is involved in DNA damage processing and maintenance of genomic stability in mammalian cells

Author

Stephen C. West, Mary Ellen Moynahan, M. Prakash Hande, Bénédicte Lemmers, Peter McPherson, Amro Shehabeldin, Cheryl H. Arrowsmith, Richard Chahwan, Razqallah Hakem, Jacinth Abraham, Roland Kanaar, Charly Chahwan, Jeroen Essers, Alberto Ciccia, Aik Kia Khaw, Maria Jasin, Rob C. Laister, Katsuhiro Hanada, Molecular Genetics, Institut de Génétique Moléculaire de Montpellier (IGMM), Centre National de la Recherche Scientifique (CNRS)-Université de Montpellier (UM), University of Zurich, and Hakem, Razqallah

Subjects

DNA re-replication, Saccharomyces cerevisiae Proteins, DNA Repair, DNA damage, DNA repair, Molecular Sequence Data, 610 Medicine & health, [SDV.CAN]Life Sciences [q-bio]/Cancer, Eukaryotic DNA replication, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, 10263 Institute of Experimental Immunology, DNA polymerase delta, Genomic Instability, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, 1300 General Biochemistry, Genetics and Molecular Biology, 2400 General Immunology and Microbiology, Chromosomal Instability, 1312 Molecular Biology, Animals, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Amino Acid Sequence, Molecular Biology, Replication protein A, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, 0303 health sciences, Endodeoxyribonucleases, General Immunology and Microbiology, Stem Cells, [SDV.BA]Life Sciences [q-bio]/Animal biology, General Neuroscience, DNA replication, 2800 General Neuroscience, Articles, Endonucleases, Molecular biology, DNA-Binding Proteins, 030220 oncology & carcinogenesis, 570 Life sciences, biology, [SDV.IMM]Life Sciences [q-bio]/Immunology, Schizosaccharomyces pombe Proteins, Homologous recombination, Sister Chromatid Exchange, DNA Damage

Abstract

Yeast and human Eme1 protein, in complex with Mus81, constitute an endonuclease that cleaves branched DNA structures, especially those arising during stalled DNA replication. We identified mouse Eme1, and show that it interacts with Mus81 to form a complex that preferentially cleaves 3′‐flap structures and replication forks rather than Holliday junctions in vitro . We demonstrate that Eme1 −/− embryonic stem (ES) cells are hypersensitive to the DNA cross‐linking agents mitomycin C and cisplatin, but only mildly sensitive to ionizing radiation, UV radiation and hydroxyurea treatment. Mammalian Eme1 is not required for the resolution of DNA intermediates that arise during homologous recombination processes such as gene targeting, gene conversion and sister chromatid exchange (SCE). Unlike Blm‐deficient ES cells, increased SCE was seen only following induced DNA damage in Eme1‐deficient cells. Most importantly, Eme1 deficiency led to spontaneous genomic instability. These results reveal that mammalian Eme1 plays a key role in DNA repair and the maintenance of genome integrity.

Published

2003

35. Overlapping hotspots in CDRs are critical sites for V region diversification

Author

Xiaohua Wang, Shanzhi Wang, Lirong Wei, Myron F. Goodman, Aviv Bergman, Matthew D. Scharff, Richard Chahwan, Thomas MacCarthy, Phuong Pham, University of Zurich, and Scharff, Matthew D

Subjects

Immunoglobulin Variable Region, Somatic hypermutation, 610 Medicine & health, Complementarity determining region, Biology, 10263 Institute of Experimental Immunology, medicine.disease_cause, Deep sequencing, Cell Line, Affinity maturation, chemistry.chemical_compound, Cytidine Deaminase, medicine, Humans, Polymerase, DNA Primers, Genetics, 1000 Multidisciplinary, Mutation, Multidisciplinary, Base Sequence, DNA, Cytidine deaminase, Complementarity Determining Regions, PNAS Plus, chemistry, biology.protein, 570 Life sciences, biology

Abstract

Activation-induced deaminase (AID) mediates the somatic hypermutation (SHM) of Ig variable (V) regions that is required for the affinity maturation of the antibody response. An intensive analysis of a published database of somatic hypermutations that arose in the IGHV3-23*01 human V region expressed in vivo by human memory B cells revealed that the focus of mutations in complementary determining region (CDR)1 and CDR2 coincided with a combination of overlapping AGCT hotspots, the absence of AID cold spots, and an abundance of polymerase eta hotspots. If the overlapping hotspots in the CDR1 or CDR2 did not undergo mutation, the frequency of mutations throughout the V region was reduced. To model this result, we examined the mutation of the human IGHV3-23*01 biochemically and in the endogenous heavy chain locus of Ramos B cells. Deep sequencing revealed that IGHV3-23*01 in Ramos cells accumulates AID-induced mutations primarily in the AGCT in CDR2, which was also the most frequent site of mutation in vivo. Replacing the overlapping hotspots in CDR1 and CDR2 with neutral or cold motifs resulted in a reduction in mutations within the modified motifs and, to some degree, throughout the V region. In addition, some of the overlapping hotspots in the CDRs were at sites in which replacement mutations could change the structure of the CDR loops. Our analysis suggests that the local sequence environment of the V region, and especially of the CDR1 and CDR2, is highly evolved to recruit mutations to key residues in the CDRs of the IgV region.

Published

2015

36. Somatic Hypermutation

Author

Jahan Yar Parsa, Matthew D. Scharff, Alberto Martin, Richard Chahwan, University of Zurich, Honjo, T, Reth, M, Radbruch, Andreas, Alt, FW, and Martin, Alberto

Subjects

Genetics, Mutation, biology, Somatic hypermutation, 610 Medicine & health, Cytidine deaminase, 10263 Institute of Experimental Immunology, medicine.disease_cause, Affinity maturation, Antigen, 1300 General Biochemistry, Genetics and Molecular Biology, MSH2, Activation-induced (cytidine) deaminase, biology.protein, medicine, 570 Life sciences, DNA mismatch repair

Abstract

V(D)J recombination produces a large repertoire of antibodies that can recognize diverse antigens. However, this repertoire is typically composed of antibodies that recognize their specific antigen with affinities that are too low to ensure the efficient clearance of infecting agents. To produce antibodies with higher affinity and sometimes changes in fine specificity, B-cells undergo a second antibody diversification process that in mice, humans, and many other species is called somatic hypermutation (SHM). Somatic hypermutation is initiated by and requires activation-induced cytidine deaminase, which converts pyrimidine (dC) to uridine (dU) on single-stranded DNA. The resulting dU:dG recruits noncanonical, error-prone forms of both base excision and mismatch repair to expand the process of SHM to include mutations in A:T as well as G:C base pairs. This ensemble of a highly mutagenic enzyme and subsequent error-prone repair results in the mutation of antibody V regions at about a million times higher frequency than occurs in other genes and is unique to antibody-forming B-cells.

Published

2015

37. Contributors

Author

Frederick W. Alt, Radbruch Andreas, Nasim A. Begum, Michael C. Carroll, Andrea Cerutti, Richard Chahwan, Tsutomu Chiba, Max D. Cooper, Riccardo Dalla-Favera, Van Duc Dang, Sabyasachi Das, Betty Diamond, Anne Durandy, Sidonia Fagarasan, Ann J. Feeney, Marc Feldmann, Simon Fillatreau, Alain Fischer, Jennifer L. Gommerman, Carl S. Goodyear, James Hagman, Richard R. Hardy, Anja E. Hauser, Kyoko Hayakawa, Barton F. Haynes, Brantley R. Herrin, Falk Hiepe, Masaki Hikida, Ellen Hilgenberg, Masayuki Hirano, Tasuku Honjo, Uta E. Höpken, Ellen Hsu, Hassan Jumaa, John F. Kearney, Garnett Kelsoe, Tadamitsu Kishimoto, Maki Kobayashi, Sven Kracker, Tomohiro Kurosaki, Marie-Paule Lefranc, Susanna M. Lewis, Jianxu Li, Andreia C. Lino, Alicia J. Little, Joseph S. Lucas, Fabienne Mackay, Giuliana Magri, Alberto Martin, Hiroyuki Marusawa, John R. Mascola, Adam Matthews, Iain B. McInnes, Fei-Long Meng, Byoung-Gon Moon, Stefan A. Muljo, Cornelis Murre, Gary J. Nabel, Hitoshi Nagaoka, Masashi Narazaki, Falk Nimmerjahn, Lars Nitschke, Alberto Nobrega, Marjorie Oettinger, Jahan Yar Parsa, Laura Pasqualucci, Klaus Rajewsky, Jeffrey V. Ravetch, Michael Reth, Roy Riblet, Stefanie Ries, David B. Roth, Imme Sakwa, Kevin O. Saunders, Matthew D. Scharff, David G. Schatz, Harry W. Schroeder, Ping Shen, Susan A. Shinton, Akritee Shrestha, Yoichi Sutoh, Atsushi Takai, Toshitada Takemori, Toshio Tanaka, David Tarlinton, Ming Tian, Alexander Tsoukas, Andre M. Vale, Markus Werner, Duane R. Wesemann, Yan Zhou, and Yong-Rui Zou

Published

2015

38. PCR-Based Detection, Restriction Endonuclease Analysis, and Transcription of tonB in Haemophilus influenzae and Haemophilus parainfluenzae Isolates Obtained from Children Undergoing Tonsillectomy and Adenoidectomy

Author

Nabil Fuleihan, Marwan Uwaydah, Ghassan M. Matar, Richard Chahwan, and Usamah Hadi

Subjects

Microbiology (medical), XhoI, biology, Clinical Biochemistry, Immunology, Virulence, biology.organism_classification, medicine.disease_cause, Molecular biology, Haemophilus influenzae, Microbiology, Chocolate agar, chemistry.chemical_compound, Endonuclease, Restriction enzyme, Restriction map, chemistry, Haemophilus parainfluenzae, biology.protein, medicine, Immunology and Allergy

Abstract

We developed and evaluated a PCR-based-restriction endonuclease analysis method to detect and analyze the tonB gene of Haemophilus influenzae and Haemophilus parainfluenzae from pediatric patients undergoing tonsillectomy and adenoidectomy. Multiple sites from the same patient, including the surface of adenoids and tonsils, as well as the core of tonsils, were cultured on chocolate agar and identified using standard procedures and the API NH Kit. A total of 55 H. influenzae isolates were recovered from different sites of 20 patients, and 32 H. parainfluenzae isolates were recovered from various sites of 12 patients. DNA was extracted from American Type Culture Collection strains and test isolates by the PureGene kit. Two primers, G1 (21-mer) and G2 (23-mer), were designed by us to amplify by PCR the tonB gene that consists of an 813-bp fragment. A nested PCR using primers T1 (23-mer) and T2 (24-mer) that flank an internal sequence to the gene of the order of 257 bp and restriction endonuclease digestion using Xho I and Bgl II were done to detect whether heterogeneity within the gene exists between the two species. Reverse transcription-PCR (RT-PCR) was finally done to detect transcription of the gene in both species. Our data have shown that the tonB gene was detected in both species. It is known to encode a virulent protein, TonB, in H. influenzae ; however, demonstration of its presence in H. parainfluenzae is novel. Nested-PCR and restriction endonuclease analysis have shown that the tonB gene is apparently structurally the same in both species, with possible differences that may exist in certain H. parainfluenzae isolates. RT-PCR done on selected numbers of H. influenzae and H. parainfluenzae have shown that the tonB gene was transcribed in both species. This shows that the TonB protein, if expressed, may play a different role in the virulence in H. parainfluenzae since it is not needed for heme or heme complexes uptake as with H. influenzae.

Published

2001

39. Mammalian Exo1 encodes both structural and catalytic functions that play distinct roles in essential biological processes

Author

Robert L. Eoff, Rani S. Sellers, Elena Avdievich, Winfried Edelmann, Sonja Schaetzlein, Richard Chahwan, Thomas A. Kunkel, Alan B. Clark, Kaichun Wei, Sergio Roa, and Matthew D. Scharff

Subjects

Exonuclease, Male, DNA End-Joining Repair, Mice, 129 Strain, DNA repair, DNA damage, Molecular Sequence Data, Biology, medicine.disease_cause, DNA Mismatch Repair, Exonuclease 1, Mice, medicine, Animals, Amino Acid Sequence, Mice, Knockout, Mutation, Multidisciplinary, Sequence Homology, Amino Acid, Mutagenesis, Mice, Mutant Strains, Mice, Inbred C57BL, Meiosis, DNA Repair Enzymes, Exodeoxyribonucleases, Biochemistry, Amino Acid Substitution, PNAS Plus, biology.protein, Mutagenesis, Site-Directed, DNA mismatch repair, Female, Mutant Proteins

Abstract

Mammalian Exonuclease 1 (EXO1) is an evolutionarily conserved, multifunctional exonuclease involved in DNA damage repair, replication, immunoglobulin diversity, meiosis, and telomere maintenance. It has been assumed that EXO1 participates in these processes primarily through its exonuclease activity, but recent studies also suggest that EXO1 has a structural function in the assembly of higher-order protein complexes. To dissect the enzymatic and nonenzymatic roles of EXO1 in the different biological processes in vivo, we generated an EXO1-E109K knockin (Exo1(EK)) mouse expressing a stable exonuclease-deficient protein and, for comparison, a fully EXO1-deficient (Exo1(null)) mouse. In contrast to Exo1(null/null) mice, Exo1(EK/EK) mice retained mismatch repair activity and displayed normal class switch recombination and meiosis. However, both Exo1-mutant lines showed defects in DNA damage response including DNA double-strand break repair (DSBR) through DNA end resection, chromosomal stability, and tumor suppression, indicating that the enzymatic function is required for those processes. On a transformation-related protein 53 (Trp53)-null background, the DSBR defect caused by the E109K mutation altered the tumor spectrum but did not affect the overall survival as compared with p53-Exo1(null) mice, whose defects in both DSBR and mismatch repair also compromised survival. The separation of these functions demonstrates the differential requirement for the structural function and nuclease activity of mammalian EXO1 in distinct DNA repair processes and tumorigenesis in vivo.

Published

2013

40. The ATPase activity of MLH1 is required to orchestrate DNA double-strand breaks and end processing during class switch recombination

Author

Johanna van Oers, Richard Chahwan, Sergio Roa, Matthew D. Scharff, Chunfang Zhao, Winfried Edelmann, and Elena Avdievich

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, DNA End-Joining Repair, DNA Repair, DNA repair, Upstream and downstream (transduction), Immunology, Somatic hypermutation, Biology, medicine.disease_cause, 03 medical and health sciences, Mice, medicine, Immunology and Allergy, Animals, DNA Breaks, Double-Stranded, neoplasms, 030304 developmental biology, Adaptor Proteins, Signal Transducing, Genetics, Adenosine Triphosphatases, Recombination, Genetic, 0303 health sciences, Mutation, B-Lymphocytes, 030302 biochemistry & molecular biology, Brief Definitive Report, nutritional and metabolic diseases, Nuclear Proteins, Cytidine deaminase, Immunoglobulin Class Switching, digestive system diseases, Non-homologous end joining, Immunoglobulin class switching, DNA mismatch repair, Somatic Hypermutation, Immunoglobulin, MutL Protein Homolog 1

Abstract

MLH1 ATPase activity is essential for class switch recombination but not for somatic hypermutation., Antibody diversification through somatic hypermutation (SHM) and class switch recombination (CSR) are similarly initiated in B cells with the generation of U:G mismatches by activation-induced cytidine deaminase but differ in their subsequent mutagenic consequences. Although SHM relies on the generation of nondeleterious point mutations, CSR depends on the production of DNA double-strand breaks (DSBs) and their adequate recombination through nonhomologous end joining (NHEJ). MLH1, an ATPase member of the mismatch repair (MMR) machinery, is emerging as a likely regulator of whether a U:G mismatch progresses toward mutation or DSB formation. We conducted experiments on cancer modeled ATPase-deficient MLH1G67R knockin mice to determine the function that the ATPase domain of MLH1 mediates in SHM and CSR. Mlh1GR/GR mice displayed a significant decrease in CSR, mainly attributed to a reduction in the generation of DSBs and diminished accumulation of 53BP1 at the immunoglobulin switch regions. However, SHM was normal in these mice, which distinguishes MLH1 from upstream members of the MMR pathway and suggests a very specific role of its ATPase-dependent functions during CSR. In addition, we show that the residual switching events still taking place in Mlh1GR/GR mice display unique features, suggesting a role for the ATPase activity of MLH1 beyond the activation of the endonuclease functions of its MMR partner PMS2. A preference for switch junctions with longer microhomologies in Mlh1GR/GR mice suggests that through its ATPase activity, MLH1 also has an impact in DNA end processing, favoring canonical NHEJ downstream of the DSB. Collectively, our study shows that the ATPase domain of MLH1 is important to transmit the CSR signaling cascade both upstream and downstream of the generation of DSBs.

Published

2012

41. Mismatch-mediated error prone repair at the immunoglobulin genes

Author

Richard Chahwan, Matthew D. Scharff, Sergio Roa, and Winfried Edelmann

Subjects

DNA Repair, DNA repair, Mismatch repair complex, Somatic hypermutation, DNA Mismatch Repair, Antibodies, Article, Mice, Cytidine Deaminase, Activation-induced (cytidine) deaminase, Animals, Humans, Pharmacology, Genetics, Mice, Knockout, biology, Genes, Immunoglobulin, Antibody Diversity, General Medicine, Cytidine deaminase, Cell biology, DNA-Binding Proteins, DNA Repair Enzymes, Immunoglobulin class switching, Mutation, biology.protein, DNA mismatch repair

Abstract

The generation of effective antibodies depends upon somatic hypermutation (SHM) and class-switch recombination (CSR) of antibody genes by activation induced cytidine deaminase (AID) and the subsequent recruitment of error prone base excision and mismatch repair. While AID initiates and is required for SHM, more than half of the base changes that accumulate in V regions are not due to the direct deamination of dC to dU by AID, but rather arise through the recruitment of the mismatch repair complex (MMR) to the U:G mismatch created by AID and the subsequent perversion of mismatch repair from a high fidelity process to one that is very error prone. In addition, the generation of double-strand breaks (DSBs) is essential during CSR, and the resolution of AID-generated mismatches by MMR to promote such DSBs is critical for the efficiency of the process. While a great deal has been learned about how AID and MMR cause hypermutations and DSBs, it is still unclear how the error prone aspect of these processes is largely restricted to antibody genes. The use of knockout models and mice expressing mismatch repair proteins with separation-of-function point mutations have been decisive in gaining a better understanding of the roles of each of the major MMR proteins and providing further insight into how mutation and repair are coordinated. Here, we review the cascade of MMR factors and repair signals that are diverted from their canonical error free role and hijacked by B cells to promote genetic diversification of the Ig locus. This error prone process involves AID as the inducer of enzymatically-mediated DNA mismatches, and a plethora of downstream MMR factors acting as sensors, adaptors and effectors of a complex and tightly regulated process from much of which is not yet well understood.

Published

2011

42. Crosstalk between genetic and epigenetic information through cytosine deamination

Author

Richard Chahwan, Sergio Roa, Sandeep N. Wontakal, University of Zurich, and Chahwan, Richard

Subjects

Genetics, Natural selection, Somatic cell, 610 Medicine & health, Cytidine deaminase, Biology, 10263 Institute of Experimental Immunology, Biological Evolution, Cytosine Deaminase, Epigenesis, Genetic, chemistry.chemical_compound, Crosstalk (biology), Cytosine, chemistry, 1311 Genetics, Deamination, Genetic variation, 570 Life sciences, biology, Animals, Humans, Epigenetics, Epigenesis

Abstract

Decades of work have elucidated the existence of two forms of heritable information, namely genetic and epigenetic, which are collectively referred to as the 'dual inheritance'. The underlying mechanisms behind these two modes of inheritance have so far remained distinct. Cytosine deaminases, such as activation-induced cytidine deaminase (AID) and other members of the APOBEC family, have been implicated both in genetic variation of somatic cells and in epigenetic remodeling of germ and pluripotent cells. We hereby synthesize these seemingly dissociated functions into one coherent model, and further suggest that cytosine deaminases, particularly AID, might have a broader influence by modulating epigenetic information in somatic or cancer cells, as well as by triggering genetic variation in germ and pluripotent cells through mutation followed by natural selection. We therefore propose that the AID/APOBEC family of deaminases are likely to have acted as drivers throughout vertebrate evolution.

Published

2010

43. The RNF8/RNF168 ubiquitin ligase cascade facilitates class switch recombination

Author

Matthew D. Scharff, Stephanie Panier, Rajeev M. Nepal, Shaliny Ramachandran, Alberto Martin, Richard Chahwan, Sergio Roa, Darina Frieder, Daniel Durocher, Ahmad Zaheen, and University of Zurich

Subjects

DNA damage, Ubiquitin-Protein Ligases, 610 Medicine & health, chemical and pharmacologic phenomena, 10263 Institute of Experimental Immunology, Cell Line, Mice, Ubiquitin, Cytidine Deaminase, Activation-induced (cytidine) deaminase, Animals, Humans, Recombination, Genetic, 1000 Multidisciplinary, Multidisciplinary, biology, Reverse Transcriptase Polymerase Chain Reaction, Intracellular Signaling Peptides and Proteins, Ubiquitination, Cytidine deaminase, Biological Sciences, Molecular biology, Ubiquitin ligase, Immunoglobulin A, DNA-Binding Proteins, Immunoglobulin class switching, biology.protein, Mdm2, 570 Life sciences, Tumor Suppressor p53-Binding Protein 1

Abstract

An effective immune response requires B cells to produce several classes of antibodies through the process of class switch recombination (CSR). Activation-induced cytidine deaminase initiates CSR by deaminating deoxycytidines at switch regions within the Ig locus. This activity leads to double-stranded DNA break formation at the donor and recipient switch regions that are subsequently synapsed and ligated in a 53BP1-dependent process that remains poorly understood. The DNA damage response E3 ubiquitin ligases RNF8 and RNF168 were recently shown to facilitate recruitment of 53BP1 to sites of DNA damage. Here we show that the ubiquitination pathway mediated by RNF8 and RNF168 plays an integral part in CSR. Using the CH12F3-2 mouse B cell line that undergoes CSR to IgA at high rates, we demonstrate that knockdown of RNF8, RNF168, and 53BP1 leads to a significant decrease in CSR. We also show that 53BP1-deficient CH12F3-2 cells are protected from apoptosis mediated by the MDM2 inhibitor Nutlin-3. In contrast, deficiency in either E3 ubiquitin ligase does not protect cells from Nutlin-3–mediated apoptosis, indicating that RNF8 and RNF168 do not regulate all functions of 53BP1.

Published

2010

44. Orchestration of the DNA-damage response by the RNF8 ubiquitin ligase

Author

Frédéric D. Sweeney, Timothy M. Thomson, Laurence Pelletier, Stephanie Panier, Jarkko Ylanko, Shinichiro Nakada, Jan Wildenhain, Nadine K. Kolas, Megan Mendez, Richard Chahwan, J. Ross Chapman, Daniel Durocher, Stephen P. Jackson, University of Zurich, and Jackson, Stephen P

Subjects

DNA Repair, DNA repair, DNA damage, Ubiquitin-Protein Ligases, Amino Acid Motifs, Molecular Sequence Data, Cell Cycle Proteins, 610 Medicine & health, Ataxia Telangiectasia Mutated Proteins, Ubiquitin-conjugating enzyme, Protein Serine-Threonine Kinases, 10263 Institute of Experimental Immunology, Article, Ubiquitin, Cell Line, Tumor, Humans, DNA Breaks, Double-Stranded, Amino Acid Sequence, Phosphorylation, RNA, Small Interfering, Adaptor Proteins, Signal Transducing, 1000 Multidisciplinary, Multidisciplinary, biology, BRCA1 Protein, Tumor Suppressor Proteins, Intracellular Signaling Peptides and Proteins, Ubiquitination, Nuclear Proteins, G2-M DNA damage checkpoint, Molecular biology, Cell Nucleus Structures, Ubiquitin ligase, MDC1, Protein Structure, Tertiary, DNA-Binding Proteins, Ubiquitin-Conjugating Enzymes, biology.protein, Trans-Activators, 570 Life sciences, Tumor Suppressor p53-Binding Protein 1, HeLa Cells

Abstract

Cells respond to DNA double-strand breaks by recruiting factors such as the DNA-damage mediator protein MDC1, the p53-binding protein 1 (53BP1), and the breast cancer susceptibility protein BRCA1 to sites of damaged DNA. Here, we reveal that the ubiquitin ligase RNF8 mediates ubiquitin conjugation and 53BP1 and BRCA1 focal accumulation at sites of DNA lesions. Moreover, we establish that MDC1 recruits RNF8 through phosphodependent interactions between the RNF8 forkhead-associated domain and motifs in MDC1 that are phosphorylated by the DNA-damage activated protein kinase ataxia telangiectasia mutated (ATM). We also show that depletion of the E2 enzyme UBC13 impairs 53BP1 recruitment to sites of damage, which suggests that it cooperates with RNF8. Finally, we reveal that RNF8 promotes the G 2 /M DNA damage checkpoint and resistance to ionizing radiation. These results demonstrate how the DNA-damage response is orchestrated by ATM-dependent phosphorylation of MDC1 and RNF8-mediated ubiquitination.

Published

2007

45. DNA-based subtypes and antimicrobial susceptibility profiles of Haemophilus influenzae and Haemophilus parainfluenzae isolated from different tonsillar sites of children undergoing tonsillectomy and/or adenoidectomy

Author

Ghassan M, Matar, Richard, Chahwan, Nabil, Fuleihan, Marwan, Uwaydah, Michel, El-Hajj, and Usamah, Hadi

Subjects

DNA, Bacterial, Male, Adolescent, Hypertrophy, Microbial Sensitivity Tests, Haemophilus influenzae, Anti-Bacterial Agents, Adenoidectomy, Tonsillitis, Child, Preschool, Drug Resistance, Bacterial, Humans, Female, Child, Haemophilus parainfluenzae, Tonsillectomy

Abstract

We did a comparative analysis between DNA-based subtypes and antimicrobial susceptibility profiles on Haemophilus influenzae and Haemophilus parainfluenzae, isolated from multiple tonsillar sites per individual from patients with chronic recurrent tonsillitis and/or tonsillar idiopathic hypertrophy and undergoing tonsillectomy and/or adenoidectomy. A total of eighty-eight Haemophilus isolates were obtained aseptically from the surface and core of tonsils and/or adenoids of 32 out of 60 patients and identified at the species level by the X and V factors and the API NH Kit. The H. influenzae and H. parainfluenzae isolates as well as ATCC strains were tested for antimicrobial susceptibility using a panel of antimicrobial agents. Random amplified polymorphic DNA (RAPD) was done on extracted DNA from all Haemophilus isolates and ATCC strains, using one 10 mer and one 18 mer primers to subtype the two species. Antimicrobial susceptibility testing data have shown a variation in generated susceptibility patterns to tested antimicrobial agents among H. influenzae and H. parainfluenzae isolates. This variation was demonstrated too among isolates obtained from different tonsillar sites (core and surface) in a single patient. RAPD analysis identified 58/88 (66%) different RAPD patterns. Variations in RAPD patterns among H. influenzae and H. parainfluenzae were also observed in isolates obtained from different tonsillar sites of the same individual. A correlation between RAPD patterns and antimicrobial susceptibility data, have shown: 1) the predominance of one strain (RAPD pattern) of either Haemophilus species among isolated organisms per patient, and exhibiting different antimicrobial susceptibility profiles or 2) the existence of multiple strains (RAPD patterns) of either Haemophilis species per patient, and showing either a single or multiple antimicrobial susceptibility profile(s). These observations question the validity of swab cultures obtained from a single tonsillar site per patient, for detection, identification and determination of antimicrobial profiles of the etiology of tonsillitis, since swab specimens taken from only one site may or may not reflect the etiology of infection.

Published

2004

46. Involvement of Mammalian Mus81 in Genome Integrity and Tumor Suppression

Author

Bénédicte Lemmers, Richard Chahwan, Roland Kanaar, M. Prakash Hande, Rama Khokha, Anuradha Poonepalli, Mary Ellen Moynahan, Otto Sanchez-Sweatman, Maria Jasin, Ashwin Pamidi, Jeroen Essers, John Peter McPherson, Razqallah Hakem, Eva Migon, Katsuhiro Hanada, Elzbieta Matysiak-Zablocki, Institut de Génétique Moléculaire de Montpellier (IGMM), Centre National de la Recherche Scientifique (CNRS)-Université de Montpellier (UM), University of Zurich, Hakem, Razqallah, and Molecular Genetics

Subjects

Lymphoma, T-Lymphocytes, 10263 Institute of Experimental Immunology, Mice, Endonuclease, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, ComputingMilieux_MISCELLANEOUS, Recombination, Genetic, 0303 health sciences, Genome, Multidisciplinary, biology, Stem Cells, [SDV.BA]Life Sciences [q-bio]/Animal biology, Gene targeting, MUS81, DNA-Binding Proteins, Meiosis, 030220 oncology & carcinogenesis, Gene Targeting, [SDV.IMM]Life Sciences [q-bio]/Immunology, Heterozygote, Saccharomyces cerevisiae Proteins, Tumor suppressor gene, Mitomycin, 610 Medicine & health, [SDV.CAN]Life Sciences [q-bio]/Cancer, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Genomic Instability, Embryonic and Fetal Development, 03 medical and health sciences, Animals, Genetic Predisposition to Disease, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Alleles, 030304 developmental biology, Chromosome Aberrations, 1000 Multidisciplinary, Mitomycin C, Embryo, Mammalian, Endonucleases, Molecular biology, chemistry, Gamma Rays, biology.protein, 570 Life sciences, Homologous recombination, Sister Chromatid Exchange, DNA, DNA Damage

Abstract

Mus81-Eme1 endonuclease has been implicated in the rescue of stalled replication forks and the resolution of meiotic recombination intermediates in yeast. We used gene targeting to study the physiological requirements of Mus81 in mammals. Mus81 –/– mice are viable and fertile, which indicates that mammalian Mus81 is not essential for recombination processes associated with meiosis. Mus81-deficient mice and cells were hypersensitive to the DNA cross-linking agent mitomycin C but not to γ-irradiation. Remarkably, both homozygous Mus81 –/– and heterozygous Mus81 +/– mice exhibited a similar susceptibility to spontaneous chromosomal damage and a profound and equivalent predisposition to lymphomas and other cancers. These studies demonstrate a critical role for the proper biallelic expression of the mammalian Mus81 in the maintenance of genomic integrity and tumor suppression.

Published

2004

47. RNF8 links nucleosomal and cytoskeletal ubiquitylation of higher order protein structures

Author

Takahiro Matsusaka, Serge Gravel, Stephen P. Jackson, Richard Chahwan, University of Zurich, and Jackson, Stephen P

Subjects

Saccharomyces cerevisiae Proteins, Ubiquitin-Protein Ligases, Mitosis, cytokinesis, Cell Cycle Proteins, 610 Medicine & health, Saccharomyces cerevisiae, Biology, 10263 Institute of Experimental Immunology, Septin, RNF8, Dma1, 1309 Developmental Biology, 1307 Cell Biology, Cell Cycle News & Views, Dma2, Protein structure, Cell Line, Tumor, ubiquitin, Schizosaccharomyces, 1312 Molecular Biology, Humans, histone modification, Histone octamer, Septin-filament, RNA, Small Interfering, Cell Cycle Protein, Cytoskeleton, Molecular Biology, Centrosome, Cell Cycle, Ubiquitination, Cell Biology, E3 ubiquitin-ligase, Ubiquitin ligase, Cell biology, DNA-Binding Proteins, Histone, biology.protein, 570 Life sciences, biology, RNA Interference, Schizosaccharomyces pombe Proteins, Septins, Cell Division, Cytokinesis, HeLa Cells, Developmental Biology

Abstract

The budding yeast proteins Dma1 and Dma2 are members of the unique FHA-RING domain protein family and are linked to mitotic regulation and septin organization by ill-defined mechanisms. We show that Dma2 has ubiquitin ligase activity, and that septins Shs1 and Cdc11 are likely direct in vivo targets. We further propose that human RNF8, rather than Chfr, is the mammalian Dma homolog. As in yeast, RNF8 localizes to the centrosomes and cell division sites and promotes ubiquitylation of the septin SEPT7, whose depletion increases cell division anomalies. Together, these findings reveal evolutionary and functional conservation of Dma proteins, and suggest that RNF8 maintains genome stability through independent, yet analogous, nuclear and cytoplasmic ubiquitylation activities.

Published

2013

48. Eme1 is involved in DNA damage processing and maintenance of genomic stability in mammalian cells.

Author

Jacinth Abraham, Bénédicte Lemmers, M.Prakash Hande, Mary Ellen Moynahan, Charly Chahwan, Alberto Ciccia, Jeroen Essers, Katsuhiro Hanada, Richard Chahwan, Aik Kia Khaw, Peter McPherson, Amro Shehabeldin, Rob Laister, Cheryl Arrowsmith, Roland Kanaar, Stephen C. West, Maria Jasin, and Razqallah Hakem

Subjects

PROTEINS, YEAST, DNA damage, MITOMYCIN C

Abstract

Yeast and human Eme1 protein, in complex with Mus81, constitute an endonuclease that cleaves branched DNA structures, especially those arising during stalled DNA replication. We identified mouse Eme1, and show that it interacts with Mus81 to form a complex that preferentially cleaves 3′-flap structures and replication forks rather than Holliday junctions in vitro. We demonstrate that Eme1-/- embryonic stem (ES) cells are hypersensitive to the DNA cross-linking agents mitomycin C and cisplatin, but only mildly sensitive to ionizing radiation, UV radiation and hydroxyurea treatment. Mammalian Eme1 is not required for the resolution of DNA intermediates that arise during homologous recombination processes such as gene targeting, gene conversion and sister chromatid exchange (SCE). Unlike Blm-deficient ES cells, increased SCE was seen only following induced DNA damage in Eme1-deficient cells. Most importantly, Eme1 deficiency led to spontaneous genomic instability. These results reveal that mammalian Eme1 plays a key role in DNA repair and the maintenance of genome integrity. [ABSTRACT FROM AUTHOR]

Published

2003